Methylation of the 4q35 D4Z4 repeat defines disease status in facioscapulohumeral muscular dystrophy

Erdmann, Hannes; Scharf, Florentine; Gehling, Stefanie; Benet‐Pagès, Anna; Jakubiczka, Sibylle; Becker, Kerstin; Seipelt, Maria; Kleefeld, Felix; Knop, Karl Christian; Prott, Eva Christina; Hiebeler, Miriam; Montagnese, Federica; Gläser, Dieter; Vorgerd, Matthias; Hagenacker, Tim; Walter, Maggie C.; Reilich, Peter; Neuhann, Teresa; Zenker, Martin; Holinski‐Feder, Elke; Schoser, Benedikt G. H.; Schöser, Benedikt

doi:10.1093/brain/awac336

Cited by 18 publications

(20 citation statements)

References 72 publications

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“…By this way, they reported a reduced average methylation of the detected CpG sites in FSHD subjects, which is in accordance with our data. Moreover, they found the association of these methylation profiles with the disease severity, as also reported by previous studies, and propose the application of DNA methylation into the diagnostic workflow [ 19 ].…”

Section: Discussionsupporting

confidence: 72%

“…Indeed, both samples referred to patients harboring a 4qA/4qA genotype, which could overestimate the methylation levels due to the fact that the assay would detect the methylation levels of both alleles, in contrast to subjects with a single copy of 4qA that would provide a more precise measure. Of note, this similar issue has also been highlighted in the recent study by Erdmann et al, 2022 [ 19 ].…”

Section: Discussionsupporting

confidence: 67%

“…Indeed, various studies investigated the association of reduced D4Z4 methylation levels with the disease, though reporting variable results depending on different sample sizes, employed methodologies (BSS, long read sequencing, antibody-based methods and utilization of methylation-sensitive restriction enzymes) and analyzed region/CpG sites (whole D4Z4 unit, 5′ DUX4 -ORF, distal region of 4q35) [ 13 , 14 , 15 , 16 , 17 , 18 , 21 , 29 ]. On this subject, the study by Erdmann et al, 2022 performed an evaluation of D4Z4 methylation in a diagnostic workflow aimed at enhancing the interpretation of disease manifestations [ 19 ]. Importantly, the study is based on a BSS-NGS approach, focusing their attention on the 4q distal region and the entire repeated unit.…”

Section: Discussionmentioning

confidence: 99%

“…Considering that the DNA methylation status representative of D4Z4 locus has been recognized as a hallmark of the disease, several research studies tested it as a possible diagnostic biomarker. In particular, a number of protocols have been proposed to assess the methylation status, although different CpG sites/regions, biological sources and variable sample sizes have been used [ 13 , 14 , 15 , 16 , 17 , 18 , 19 , 20 , 21 ]. Given these premises, mathylation analysis and Machine Learning (ML) pipelines were tested as possible methods to prioritize FSHD subjects for standard molecular testing and supporting the clinical diagnosis.…”

Section: Introductionmentioning

confidence: 99%

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D4Z4 Methylation Levels Combined with a Machine Learning Pipeline Highlight Single CpG Sites as Discriminating Biomarkers for FSHD Patients

Caputo

Megalizzi

Fabrizio

et al. 2022

Cells

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The study describes a protocol for methylation analysis integrated with Machine Learning (ML) algorithms developed to classify Facio-Scapulo-Humeral Dystrophy (FSHD) subjects. The DNA methylation levels of two D4Z4 regions (DR1 and DUX4-PAS) were assessed by an in-house protocol based on bisulfite sequencing and capillary electrophoresis, followed by statistical and ML analyses. The study involved two independent cohorts, namely a training group of 133 patients with clinical signs of FSHD and 150 healthy controls (CTRL) and a testing set of 27 FSHD patients and 25 CTRL. As expected, FSHD patients showed significantly reduced methylation levels compared to CTRL. We utilized single CpG sites to develop a ML pipeline able to discriminate FSHD subjects. The model identified four CpGs sites as the most relevant for the discrimination of FSHD subjects and showed high metrics values (accuracy: 0.94, sensitivity: 0.93, specificity: 0.96). Two additional models were developed to differentiate patients with lower D4Z4 size and patients who might carry pathogenic variants in FSHD genes, respectively. Overall, the present model enables an accurate classification of FSHD patients, providing additional evidence for DNA methylation as a powerful disease biomarker that could be employed for prioritizing subjects to be tested for FSHD.

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Section: Discussionsupporting

confidence: 72%

Section: Discussionsupporting

confidence: 67%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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D4Z4 Methylation Levels Combined with a Machine Learning Pipeline Highlight Single CpG Sites as Discriminating Biomarkers for FSHD Patients

Caputo

Megalizzi

Fabrizio

et al. 2022

Cells

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“…Similar issues with inconclusive diagnostic analysis of FSHD based on detection of 4qA methylation levels have also been noted in recent studies. 21,22…”

Section: Discussionmentioning

confidence: 99%

Association of 4qA-Specific Distal D4Z4 Hypomethylation With Disease Severity and Progression in Facioscapulohumeral Muscular Dystrophy

et al. 2023

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Objective:To examine whether the regional methylation levels at the most distal D4Z4 repeat units (RU) in the 4qA-permissive haplotype were associated with disease severity and progression in facioscapulohumeral muscular dystrophy type 1 (FSHD1).Methods:This was a 21-year, retrospective, and observational cohort study conducted at the Fujian Neuromedical Centre (FNMC) in China. Methylation levels of the most distal D4Z4 RU, including 10 CpGs, were assessed in all participants by bisulfite sequencing. FSHD1 patients were stratified into 4 groups based on methylation percentage quartiles, including LM1 (low methylation), LM2 (low to intermediate methylation), LM3 (intermediate to high methylation), and highest methylation levels (HM). Patients received evaluations of motor function focusing on lower extremity (LE) progression at baseline and in follow-ups. FSHD clinical score (CS), age-corrected clinical severity scale (ACSS), and modified Rankin Scale were used to assess motor function.Results:The methylation levels of the 10 CpGs were significantly lower in all 823 genetically confirmed FSHD1 patients than in 341 healthy controls (HCs). CpG6 methylation levels could distinguish: 1) FSHD1 patients from HCs; 2) symptomatic from asymptomatic/unaffected patients; 3) patients with LE involvement from those without LE involvement, with AUCs (95% CI) of 0.9684 (0.9584–0.9785), 0.7417 (0.6903–0.7931), and 0.6386 (0.5816–0.6956), respectively. CpG6 methylation levels were negatively correlated with both CS (r = -0.392) and ACSS (r = -0.432), and positively correlated with onset age of first-ever muscle weakness (r = 0.297). For the LM1, LM2, LM3, and HM groups, the respective proportions of LE involvement were 52.9%, 44.2%, 36.9%, and 23.4%; and onset ages of LE involvement were 20, 26.5, 25, and 26.5 years. Cox regression analysis—adjusted for sex, age at examination, D4Z4 RU, and 4qA/B haplotype—showed that the LM1, LM2, and LM3 groups (i.e., groups with lower methylation levels) had a higher risk for independent ambulation loss, with HRs (95% CI) of 3.523 (1.565–7.930), 3.356 (1.458–7.727), and 2.956 (1.245–7.020), respectively.Conclusion:4q35 distal D4Z4 hypomethylation is correlated with disease severity and progression to lower extremity involvement.

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Updates on Facioscapulohumeral Muscular Dystrophy (FSHD)

Chin,

Quak,

Chan

et al. 2024

Curr Treat Options Neurol

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Methylation of the 4q35 D4Z4 repeat defines disease status in facioscapulohumeral muscular dystrophy

Cited by 18 publications

References 72 publications

D4Z4 Methylation Levels Combined with a Machine Learning Pipeline Highlight Single CpG Sites as Discriminating Biomarkers for FSHD Patients

D4Z4 Methylation Levels Combined with a Machine Learning Pipeline Highlight Single CpG Sites as Discriminating Biomarkers for FSHD Patients

Association of 4qA-Specific Distal D4Z4 Hypomethylation With Disease Severity and Progression in Facioscapulohumeral Muscular Dystrophy

Updates on Facioscapulohumeral Muscular Dystrophy (FSHD)

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